3,4-Diaminopyridine Base Effectively Treats the Weakness of Lambert-Eaton Myasthenia1
Donald B Sanders, MD1, Vern C Juel, MD
1, Yadollah Harati, MD
2, A. Gordon Smith, MD
3,
Amanda C Peltier, MD4, Tessa Marburger, MD
5, Jau-Shin Lou, MD, PhD
6, Robert M Pascuzzi,
MD7, David P Richman, MD
8, Tai Xie, PhD
9, Valentin Demmel, PhD
10, Laura R Jacobus, BA
11,
Kathy L Aleš, MD11
, David P Jacobus, MD11
and The DAPPER Study Team*
1: Department of Neurology, Duke University Medical Center, Durham, NC.
2: Department of Neurology, Baylor College of Medicine, Houston, Texas
3: Department of Neurology, University of Utah School of Medicine, Salt Lake City, UT
4: Department of Neurology, Vanderbilt Medical Center, Nashville, TN
5: Catholic Health Initiative St. Alexius Health – Williston Medical Center, Williston, ND;
formerly with Department of Neurology, Oregon Health and Science University, Portland, OR
6: Department of Neurology, University of North Dakota School of Medicine & Health Science,
Fargo, ND; formerly with Department of Neurology, Oregon Health and Science University,
Portland, OR
7: Department of Neurology, Indiana University, Indianapolis, IN
8: Department of Neurology, Center for Neuroscience, University of California, Davis, Davis,
CA
9: Brightech International LLC, Somerset, NJ
1 Presented in part at the Annual Meetings of the American Academy of Neurology, Washington, DC, April 23,
2015; the American Neurological Association, Chicago, September 28, 2015; and the American Association of
Neuromuscular & Electrodiagnostic Medicine, Honolulu, October 28, 2015.
___________________________________________________________________
This is the author's manuscript of the article published in final edited form as:Sanders, D. B., Juel, V. C., Harati, Y., Smith, A. G., Peltier, A. C., Marburger, T., Lou, J.-S., Pascuzzi, R. M., Richman, D. P., Xie, T., Demmel, V., Jacobus, L. R., Aleš, K. L., Jacobus, D. P. and The DAPPER Study Team (2018), 3,4-Diaminopyridine Base Effectively Treats the Weakness of Lambert-Eaton Myasthenia. Muscle Nerve. Accepted Author Manuscript. http://dx.doi.org/10.1002/mus.26052
3,4-DAP in LEM – Page 2
10: nabios GMBH, Munich, Germany
11: Jacobus Pharmaceutical Company, Inc., Princeton, NJ
*DAPPER Study Team:
Co-Investigators:
Jeffrey T. Guptill, MD
Janice M. Massey, MD
Lisa D. Hobson-Webb, MD
Ali Arvantaj, MD
Cecile Phan, MD
Shima Mousavi, MD
J. Robinson Singleton, MD
Peter D. Donofrio, MD
Christopher Lee, MD, MPH
Alexandra Dimitrova, MD
Brent Burroughs, MD
Ghazaleh Jafari, MD
Julie Khoury, MD
Mananya Satayaprasert, MD
Cynthia Bodkin, MD
John Kincaid, MD
Riley Snook, MD
Mark A. Agius, MD
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Study Coordinators:
Katherine Beck, RN
Claire MacAdam, PT
Charles Latner
Meg Lessard
Kay Artibee, RN MEd
Diana Dimitrova, PhD
Angela Micheels PT
Sandra Guingrich
Janelle Butters, RN
Acknowledgements:
Study Monitoring: Bradstreet Clinical Research Associates, Inc.
3TUG Blinded Readings: Ready Clinical, LLC
Statistical Consultation: Brightech International
Data Management and Statistical Services: EDETEK, Inc
CMAP Blinded Reviews: Erik Stålberg, MD, PhD, Uppsala University
ECG Analysis: nabios GMBH
Abstract word count: 149
Manuscript word count: 3,911 exclusive of references and tables
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Reprint requests: not available
Correspondence to:
Donald B. Sanders, MD
Box 3403, Duke University Medical Center, Durham, NC 27710
Email: [email protected]
Sponsor: Jacobus Pharmaceutical Co., Inc.
Author disclosures:
Drs. Sanders, Demmel and Xie are Consultants for Jacobus Pharmaceutical Co., Inc.
Laura Jacobus is Vice President, Jacobus Pharmaceutical Co., Inc.
Dr. Aleš is Medical Director, Jacobus Pharmaceutical Co., Inc.
Dr. David Jacobus is President, Jacobus Pharmaceutical Co., Inc.
The remaining authors have no conflicts of interest.
We confirm that we have read the Journal’s position on issues involved in ethical publication and
affirm that this report is consistent with those guidelines.
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ABSTRACT
Introduction: 3,4-diaminopyridine has been used to treat Lambert Eaton myasthenia (LEM) for
thirty years despite the lack of conclusive evidence of efficacy.
Methods: We conducted a randomized double-blind placebo-controlled withdrawal study in
LEM patients who had been on stable regimens of 3,4-diaminopyridine base (3,4-DAP) for ≥ 3
months. The primary efficacy endpoint was >30% deterioration in Triple Timed Up-and-Go
(3TUG) times during tapered drug withdrawal. The secondary endpoint was self-assessment of
LEM–related weakness (W-SAS).
Results: 32 participants were randomized to continuous 3,4-DAP or placebo. None of the 14
receiving continuous 3,4-DAP had >30% deterioration in 3TUG time vs 72% of the 18 who
tapered to placebo (p<0.0001). W-SAS similarly demonstrated an advantage for continuous
treatment over placebo (p<0.0001). Need for rescue and adverse events were more common in
the placebo group.
Discussion: This trial provides significant evidence of efficacy of 3,4-DAP in the maintenance
of strength in LEM.
Key Words: Lambert-Eaton myasthenia; 3,4-diaminopyridine; amifampridine; clinical trial;
efficacy; Lambert-Eaton myasthenic syndrome; Lambert-Eaton syndrome; LES; Eaton-Lambert
syndrome; LEMS; ELS; Timed Up-and-Go
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INTRODUCTION
LEM is a rare autoimmune disorder often associated with a malignancy, usually small cell lung
cancer.1
Epidemiologic studies suggest that there may now be approximately 800 patients with
LEM in the USA and up to 170 new cases annually.2,3
The symptoms that characterize LEM result from reduced release of acetylcholine (ACh)
from the presynaptic terminals of the neuromuscular junctions.1
Autoantibodies that target
presynaptic voltage-gated calcium channels (VGCCs) impair entry of calcium into nerve
terminals, thereby decreasing ACh release.4 By blocking presynaptic potassium channels, 3,4-
diaminopyridine, also known as amifampridine, prolongs depolarization from impulses arriving
at the nerve ending, allowing VGCCs to remain open longer, thus increasing entry of calcium.
Since the quantal release of ACh depends on the intracellular concentration of calcium, 3,4-
diaminopyridine increases the release of ACh.
The first use of 3,4-diaminopyridine formulated as the free base (3,4-DAP) in the
treatment of LEM was described in 19835 and subsequent uncontrolled studies reported benefits
in small numbers of patients.6 In a double-blind, placebo-controlled crossover study of 3,4-DAP
in 12 LEM patients in 1989,7 oral doses up to 100 mg/day were effective in treating both the
motor and autonomic deficits, and the amplitude of compound muscle action potentials
(CMAPs) nearly doubled. A randomized, placebo-controlled study of 26 LEM patients in 2000
demonstrated that those who received oral 3,4-DAP had a greater improvement in Quantitative
MG (QMG) score and in the summated amplitude of CMAPs in 3 sentinel muscles,8 although the
magnitude of change in QMG score in this study was not clinically significant. A randomized,
placebo-controlled crossover study demonstrated efficacy of intravenous 3,4-DAP using
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dynamometry and CMAP in 9 LEM patients.9 None of these studies was used to file for
regulatory approval in the USA or in Europe. Other clinical studies failed to provide definitive
objective evidence of efficacy of 3,4-diaminopyridine.10,
11
In 1990 the US Food and Drug Administration granted orphan designation to 3,4-
diaminopyridine, and compassionate use of the free base formulation, (3,4-DAP), became
available through physician-held INDs for named patients in the USA and through special
governmental approvals in other countries.
To provide definitive evidence of efficacy, we designed the 3,4-DAP Product Efficacy
Research (DAPPER) trial, a prospective, placebo-controlled withdrawal study of 3,4-DAP in
LEM.
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METHODS
Outcome Measures:
Because physiologic endpoints of dynamometry and CMAP do not capture function, and QMG
performance in LEM had proven questionable in previous clinical trials, we used the 3TUG
walking test, a modification of the validated Timed Up and Go test,12
as the quantitative measure
of proximal muscle function.13
Based on minimal detectable change data reported in Parkinson
disease, the primary efficacy outcome was defined as a >30% deterioration in the 3TUG
time.14,12
Study Participants:
Given the paucity of eligible subjects, we targeted LEM patients being actively treated with 3,4-
DAP, for whom responsiveness could be objectively documented before randomization.15
To be
eligible, participants had to indicate a need to wait briefly after the first morning dose of 3,4-
DAP for improvement in LEM-related dysfunction, and they also needed to display quantifiable
functional benefit after the first morning dose.15
This approach avoided entering participants
whose LEM may have improved or remitted over time.16
Fifty-two LEM patients, all participants in the Sponsor’s 3,4-DAP compassionate use
program, were screened for eligibility. Fifty of them were receiving treatment under 21 different
physician-held INDs in the USA. One participant each from Canada and Argentina had special
access through appropriate governmental agencies and local neuromuscular specialists. The
diagnosis of LEM was confirmed by independent neurologist (DBS) review of clinical records,
including VGCC antibody and electromyography test results. The dose of 3,4-DAP was at least
10 mg 3 times a day and up to a total daily dose of 100 mg, and permitted participants to walk,
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with or without an assistive device. All LEM-related treatments were stable for at least 3
months, and other concomitant medications for at least 1 month before study entry.
Patients were excluded if they had previous respiratory failure while on 3,4-DAP or an
insufficient 3TUG response to 3,4-DAP during the baseline observation period. (See eTables 1 &
2 for detailed inclusion and exclusion criteria.)
Study Oversight:
Written informed consent was obtained from all study participants. The study was conducted in
accordance with International Conference on Harmonization guidelines and principles of the
Declaration of Helsinki. The protocol was approved by the institutional review board at each
study site and registered with clinicaltrials.gov (NCT01511978).
Criteria for rescue requiring reinstitution of baseline dosing were: new dysphagia, a drop
in pulse oximetry of 5% from baseline, or a decrease in oxygen saturation to < 90% with
accompanying shortness of breath. Inability to get out of bed or inability to arise from a chair,
even with assistance, after 2 efforts about 1 hour apart, also merited reinstitution of baseline 3,4-
DAP.
Continuous safety monitoring was built into the study design, precluding the need for a
formal safety monitoring committee.
The definition for eligibility was concealed during the study. Individual 3TUG results
were shared with the Sponsor, who determined if the eligibility criterion had been met. The
initial eligibility criterion for randomization required ≥ 30% improvement in 3TUG after the first
3,4-DAP dose on 2 consecutive mornings. This criterion threshold was lowered to ≥27% after
approximately 20% of participants had been randomized due to the constrained number of
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potential participants and concern that participants who were responsive to 3,4-DAP were being
excluded. The eligibility criterion was further modified after approximately 30 to 40% of
participants had been randomized to accommodate a potential stacking effect of 3,4-DAP (i.e.,
the additive effect of multiple doses of 3,4-DAP throughout the day) and allowing consideration
of 3TUGs performed in the afternoon as well as in the morning to determine if subsequent
participants displayed a sufficiently large response to 3,4-DAP during the baseline observation
period. A later modification also permitted consideration of the evening post-dose 3TUG. The
four thresholds used for each participant are detailed in eTables 3 & 4. Each modification made
it easier for subjects to qualify for participation and less likely that they would weaken enough
during the drug taper to reach the study endpoint.
Vital signs including pulse oximetry were measured at least 6 times daily in conjunction
with 3TUG testing, with continuous pulse oximetry monitoring overnight. Post-dose W-SAS
was obtained three times daily as was an inventory of LEM-related signs or symptoms.
Electrocardiograms (ECGs) and CMAPs were obtained before and after the first doses of the
morning and afternoon throughout the study. A Lower Extremity Function Scale (LEFS) score
was obtained at baseline and at the end of the study.17
Blood for plasma drug and metabolite
levels was drawn at regular intervals surrounding doses during the baseline observation period
and after randomization.
Participants were classified into one of four baseline treatment categories according to
their baseline LEM treatment regimen: 3,4-DAP plus pyridostigmine, 3,4-DAP alone, 3,4-DAP
plus pyridostigmine plus immunomodulators/immunosuppressants, and 3,4-DAP plus
immunomodulators/ immunosuppressants. To assure that the two study arms were balanced for
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possible disease severity, participants within each category were randomized centrally in a 1:1
ratio.
Study Design (Figure 1)
A screening visit was scheduled up to 4 weeks before admission to the inpatient clinical research
unit. After determination of initial eligibility, participants were hospitalized and observed for 2.5
days on their usual dose and schedule of 3,4-DAP. Responsiveness to 3,4-DAP, the final
determinant of eligibility, was assessed by 3TUG testing before and after the first doses of the
morning, afternoon, and evening, regardless of a participant’s total number of daily doses. The 2
hour post-dose period was selected as the estimated time for peak pharmacodynamic effect.9
Because LEM patients usually do not take 3,4-DAP during the night and the half-life following
oral doses is approximately 3.5 to 4 hours, patients effectively experience a withdrawal from
drug every night and frequently have mobility issues before their first dose of the morning. This
suggested that morning would be the ideal time to detect drug responsiveness.
Subjects with a sufficient 3TUG response were randomly assigned to the taper to placebo
group or the continuous 3,4-DAP group on the afternoon of the second day.
Tapered withdrawal began with the last dose of the second full hospital day, which was
decreased to 90% of the participant’s usual dose. Each consecutive dose was then decreased so
that it was 50% of the usual dose by the end of the third full day, 20% at the end of the fourth
day and 0% for the third dose of the fifth full day (eFigure 1). Thereafter, there was an
additional up to 16 hours with no 3,4-DAP before the participant’s usual dose was restored.
Participants were then observed for 0.5 days or until deemed clinically stable, and then
discharged. Standardized weekly follow-ups continued for one month after discharge.
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Enrollment was planned to cease when approximately 15 participants were enrolled in
each of the 2 study groups.
Treatments:
The Sponsor prepared tablets of 0.5, 2, 3, 4, 5, and 10 mg 3,4-DAP and placebo, all identical
in appearance. Combinations of 4 tablets were pre-packaged into a series of blisters to
permit a smooth taper (eFigure 2) based on each participant’s individualized pre-
randomization dosing regimen.
Efficacy Endpoints:
Primary Endpoint: The primary efficacy measure was the percent change in the last
completed post-dose 3TUG during the treatment period compared with the average of the 2
time-matched 3TUGs obtained during the baseline. The 3TUG involves 3 repetitions
without rest (laps), of rising from an 18” straight-backed armchair, walking to a line 10 feet
from the chair, and returning to sit in the chair.15
Participants are instructed to walk at their
normal pace and only prompted with the word “Go” for the first lap and “Go again” after
they come to a full stop in the chair for the subsequent laps. Each lap is timed and the score
is the average of the 3 lap times. In addition to timing the 3TUGs “live” using a traceable
stop watch, the tests were videotaped and the lap times were later measured in triplicate by a
remote assessor blinded to the treatment and to the date, time, and sequence of the 3TUGs.
The blinded assessor’s times were used to determine the primary endpoint. The calculation
of percent change in 3TUG for the primary endpoint utilized the last completed post-dose
3TUG during the withdrawal period:
Percent change = 100 x [1 - (final post-dose 3TUG ⁄ time-matched baseline 3TUGs)].
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Rescue was an anticipated event and rescued participants were considered to have
completed the trial.
Secondary Endpoint: The secondary efficacy measure was the W-SAS, a 7 level
categorical scale developed by the Sponsor to demonstrate participant-perceived change in
overall strength from study entry; responses ranged from “Much Much Weaker (-3)” to “Much
Much Stronger (+3)”. The W-SAS was obtained 3 times daily corresponding to the post-
dose 3TUGs. The last completed post-dose W-SAS during the randomized treatment period
was the endpoint.
Additional Efficacy Endpoints: Change in CMAP was measured in the nerve-muscle pair
determined to be most responsive to 3,4-DAP during acclimation (ulnar nerve - abductor
digiti minimi, median nerve — abductor pollicis brevis, or peroneal nerve – extensor
digitorum brevis). A reviewer blinded to the treatment and to the date, time, and sequence
of the CMAPs used pre-determined criteria to assess CMAP test quality. Tests approved by
this reviewer were used to determine change in CMAP amplitude at the end of the blinded
treatment period compared with baseline.
The LEFS at the end of the blinded treatment period was compared with baseline. This
questionnaire consists of 20 items, each scored from 0 (extreme difficulty) to 4 (no difficulty); a
change of 9 points has been determined to represent a clinically-meaningful functional change in
subjects with a lower extremity musculoskeletal condition.17
Need for rescue was considered both as an efficacy and a safety endpoint. Blinded
physician assessment of treatment effect was performed once at the end of the study.
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Safety Endpoints: Safety assessments included need for rescue during blinded treatment
and/or the emergence of LEM-related signs and symptoms or pre-dosage LEM-associated
weakness, 3TUG, W-SAS, and treatment-emergent adverse events. Changes in ECG
parameters, vital signs and pulse oximetry were also examined.
Plasma Drug Levels: Pharmacokinetic analyses of plasma drug and metabolite levels were used
to confirm the taper.
Statistical Analysis
Setting α at 0.05 and the power at 80%, 10 participants were required in each study group. To
allow for departures in the assumptions, 30 participants were planned, 15 for each treatment arm.
Thirty-two participants were actually enrolled. No interim analysis was performed. Statistical
analyses followed the intention-to-treat principle. Fisher’s exact test was used to compare
primary efficacy outcomes between treatment groups (i.e., >30% prolongation in 3TUG times)
and t-test was used to compare W-SAS assessments. ECGs were analyzed for changes in cardiac
intervals and a concentration response analysis exploring changes in QTcF and plasma drug
concentrations was performed. Statistical analysis of the other outcome measures was not
performed.
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RESULTS
Subjects: Fifty-two subjects were screened at 7 study sites and agreed to participate
(Figure 2). Eighteen were ineligible due to insufficient improvement in 3TUG (eTable 4).
Two subjects were excluded due to positive toxicology testing. Thirty-two participants were
eligible and were randomized, 14 to continuous 3,4-DAP and 18 to taper to placebo. There
were no important differences between the two treatment groups in demographics (Table 1),
LEM-related history or LEM treatments (eTables 5 & 6). All randomized participants
completed the study.
Efficacy:
Primary Outcome Measure: >30% deterioration in final 3TUG time during tapered
withdrawal of study drug.
The 3TUG primary efficacy endpoint demonstrated a highly significant difference
between treatment groups in favor of continuous 3,4-DAP (Table 2, Figure 3). There was very
strong agreement and a high correlation between the blinded 3TUGs and the on-site 3TUGs
(correlation coefficient=0.9192, eFigure 2).
A significantly greater proportion of subjects tapered to placebo had >30% deterioration
in the final post-dose 3TUG test compared to subjects in the continuous 3,4-DAP group. Results
were consistent for efficacy, intent-to-treat, and per protocol populations.
Secondary Outcome Measure: W-SAS.
The W-SAS secondary efficacy endpoint (Table 2) also demonstrated a highly significant
difference in favor of the continuous 3,4-DAP group, with most participants who continued
3,4-DAP being “about the same” and most of those who tapered to placebo being “Much
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Weaker” or “Much Much Weaker” at the last W-SAS assessment . Results were consistent
for the efficacy, intent-to treat, and per-protocol populations.
Additional Outcome Measures
The final post-dose CMAP measurements approved by the blinded reviewer favored the
continuous 3,4-DAP group, that had a median CMAP of 3.4 mV (all nerve-muscle pairs)
and a median percentage change of -9.5 %, while the taper to placebo group, for whom the
median final CMAP was 2.3 mV, had a median percent change from baseline of -42.1%.
The continuous 3,4-DAP group had a median change in LEFS score of -1.5 points
compared with -27 points for the taper to placebo group. In a repeat LEFS assessment one week
post-discharge in the taper to placebo group, the median score increased from 10 to 42, returning
to baseline.
Two participants in the continuous treatment group (14.3%) and 5 in the taper to placebo
group (44.4%) were rescued for new dysphagia during the withdrawal phase, without reaching
the primary study endpoint (eTable 3). In addition, one participant in the tapered group was
rescued due to a 5% drop in oxygen saturation and another required rescue due to inability to rise
from a chair. Two of the seven rescued participants in the tapered group did not meet the
primary endpoint prior to rescue (eTable 3a). Another participant in the tapered group had
baseline medication reinstituted upon request due to anxiety and a sense of impending doom,
preceded by intermittent nocturnal hypoxemia.
Blinded physician assessment of treatment effect at the end of the study favored the
continuous 3,4-DAP group, with physicians indicating that 12 of 14 (86%) subjects had no
change, while 1 each was somewhat worse or much worse than during baseline. In contrast, 14
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of the 18 (78%) participants in the taper to placebo group were considered much worse, 3 (17%)
were somewhat worse, and only one had no change from baseline.
Recovery of 3TUG After Reinstitution of 3,4-DAP:
The morning post-dose 3TUG returned to baseline after reinstitution of baseline 3,4-DAP
doses in all participants who tapered to placebo and in those who were rescued or advanced
early (Figure 3).
Recovery of W-SAS After Reinstitution of 3,4-DAP:
Participants in the taper to placebo group reported return to their baseline strength after the
first dose of their baseline 3,4-DAP dosage. A similar recovery in the W-SAS assessment
was observed in rescued participants.
Unblinding:
There were no identified instances of unblinding during the study. At the end of the study,
participants and investigators were independently asked to which treatment arm they
believed they had been randomized. Participants and physicians agreed in all cases; both
guessed treatment assignment incorrectly in 3 cases.
Pharmacokinetic Results:
Pharmacokinetic sampling was assayed post hoc and confirmed the randomization. First
morning pre-dose plasma drug levels confirmed that most participants, regardless of their
treatment arm, had effectively withdrawn from drug overnight.
Safety:
Treatment-Emergent Adverse Events (TEAEs): TEAEs were reported with a higher
frequency in the taper to placebo group, with 23 AEs in 12 of the 18 participants (67%) vs 9
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in 5 of 14 participants (36%) in the continuous 3,4-DAP group. The most common non-
LEM-related signs and symptoms TEAEs were abdominal discomfort and respiratory tract
infection (2 in the taper to placebo group). One in each treatment group had back pain,
headache, nasopharyngitis, or oropharyngeal pain. One serious AE of pneumonia occurred
in a participant in the taper to placebo group more than 3 weeks after completing the
inpatient trial. There were no deaths in this study.
Re-emergence of LEM-related signs and symptoms
The most common LEM-related signs and symptoms to emerge during drug withdrawal
were decreased oxygen saturation in 3 participants in the taper to placebo group, muscle
spasms and nausea each in 2 participants in the taper to placebo group, and arthralgia, in
1 participant in each group. One participant in the taper to placebo group had a severe
episode of anxiety with a sense of impending doom.
Based on the morning pre-dose 3TUGs, participants who were not rescued were no weaker
at the end of the 3.5-day taper than they were every morning on their usual steady regimen
of 3,4-DAP.
Clinical Laboratory Tests:
With the exception of minor blood glucose increases, there were no clinically meaningful
laboratory value changes. End of Study measurements of blood glucose were increased
compared to Screening in both treatment groups, mean blood glucose being increased by
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21.3 and 15.9 mg/dL in the taper to placebo group and continuous 3,4-DAP group,
respectively.
Vital Signs:
Small increases in average pulse rate of 4 to 6 bpm were observed at some time points post-
dose in both treatment groups.
Low oxygen saturation occurred in 5 participants in the taper to placebo group and was
reported as a LEM-related sign/symptom AE in 3 participants who had pre-existing pulmonary
disease and/or sleep apnea and who received supplemental oxygen. Low oxygen saturation
resolved spontaneously or with reinstitution of 3,4-DAP treatment. Oxygen saturation did not
worsen significantly in any participant who received continuous 3,4-DAP.
ECGs:
None of the participants had clinically significant abnormal ECG findings. All ECG
parameters (RR, QRS, PR, QT and QTcF) as well as the interpretative statements by the
investigators showed little or no differences between baseline and study days or between the
treatment groups.
An increased heart rate up to 5 bpm was observed in the taper to placebo group. Short-term
withdrawal of 3,4-DAP had no apparent effect on standard ECG parameters. Linear
regression analysis indicated that there was no relationship between changes in QTcF
interval and the respective plasma drug concentrations, regardless of treatment group.
Tolerability:
3,4-DAP in doses from 30 to 100 mg daily was well-tolerated by participants in the
continuous 3,4-DAP group.
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Discussion:
This trial provides highly significant evidence of efficacy and demonstrates that 3,4-DAP is
essential for the maintenance of strength in patients with LEM. Lowering 3,4-DAP resulted in
significant deterioration of strength when doses reached approximately 50% of the usual
individual dosage (Figure 3). Rescue was required in 44% of participants who tapered 3,4-DAP
and resulted in prompt resolution of weakness.
DAPPER contained 2 embedded efficacy studies in addition to the overall
randomized withdrawal trial: (1) a series of N of 1 trials of each participant’s daily responses
to 3,4-DAP and (2) the responses to reinstitution of 3,4-DAP at the end of the study. The
recovery of strength and function with reinstitution of 3,4-DAP supports the lack of
deconditioning, rebound weakness or sustained negative effects from short-term withdrawal
of 3,4-DAP.
Key to the potential success of the withdrawal design was the identification of 3,4-DAP-
responsive LEM patients, which ensured an enriched population for the study.
While the TUG has been validated and used to study a variety of conditions, the use of 3
repetitions of the TUG for the DAPPER study was developed to accommodate the
neuromuscular fatigue or facilitation that may affect LEM patients to different degrees. Initial
pilot testing indicated the ability of the 3TUG to detect drug effect 1 to 2 hours post-dose. A
subsequent study demonstrated the reliability of the 3TUG in controls, in non-LEM patients with
neuromuscular disease and in LEM patients.13
Pharmacokinetic/pharmacodynamic analysis of
plasma levels of 3,4-DAP from the DAPPER study demonstrated a concentration-response
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3,4-DAP in LEM – Page 21
relationship with 3TUG times, supporting the use of the 3TUG as a measure of disease-related
weakness in patients with LEM.18
The 3TUG data used in the analysis of the DAPPER study were timed from videos made
on site. In order to eliminate a potential source of bias in outcome assessment, the video reader
was remote from any of the study sites and blinded to the sequence of the tests and treatment
assignments There was very strong agreement and a high correlation between the blinded
3TUGs and the on-site 3TUGs.
The study can be criticized for changing the eligibility criterion after the study had
started. However, the study endpoint was not changed and decreasing the required level of
responsiveness for eligibility to <30% should have made it less likely that participants would
have >30% deterioration when tapered to placebo. To avoid potential biasing of the 3TUG
results used to determine eligibility, site personnel were blinded to the eligibility threshold. The
Sponsor determined eligibility from data reported by the sites using pre-set criteria that were not
subject to bias.
Although only one study participant had paraneoplastic LEM (eTable 3a, Screen No.
50.0), previous reports have demonstrated clinical responsiveness to 3,4-DAP in paraneoplastic
LEM and that there is no difference in responsiveness in paraneoplastic and non-paraneoplastic
LEM.7,19
That 2 participants in the continuous 3,4-DAP treatment group were rescued for
dysphagia is evidence for the effectiveness of the blind. Both participants and study personnel
may have been overly attuned to swallowing issues, knowing that participants would be rescued
under the protocol to avoid aspiration. The onset of dysphagia in these 2 participants
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demonstrates that even with usual treatment, LEM patients may experience unexpected weakness
that can be addressed by an extra dose of 3,4-DAP.
The highly significant findings for both the primary and secondary outcome measures are
strengthened by the rapid recovery of function upon resumption of the participants‘ usual
regimens and the finding that the majority of subjects in the continuous 3,4-DAP group had daily
demonstrable benefit with >30% improvement in 3TUG times compared to the morning pre-dose
3TUG.
Conclusion
3,4-Diaminopyridine base (3,4-DAP) is safe and effective treatment for LEM-related
weakness.
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3,4-DAP in LEM – Page 23
Table 1. Demographics and Baseline Characteristics
Taper to
Placebo
Continuous
3,4-DAP base
N 18 14
Age, years, Mean (SD),
Range
59.3 (14.99)
28 - 78
50.7 (15.97)
23 - 83
Gender: Male, N (%)
Female, N (%)
7 (38.9%)
11 (61.1%)
4 (30.8%)
10 (71.4%)
Race: White, N (%)
Black, N (%)
18 (100%)
0 (0.0%)
11 (78.6%)
3 (21.4%)
Ethnicity: Hispanic or Latino, N (%)
Not Hispanic or Latino, N (%)
1 (5.6%)
17 (94.4%)
0 (0.0%)
14 (100%)
BMI, kg/m2, Mean (SD)
Range
27.7 (5.14)
18.9 - 35.4
27.3 (5.92)
20.3 - 39.0
Positive P/Q VGCC-Ab at screening, N (%) 17 (94.4%) 12 (85.7%)
CMAP facilitation >100% at Screening, N (%) 10 (55.6%) 7 (50.0%)
Paraneoplastic LEM, N (%) 1 (5.6%) 0 (0.0%)
Duration of LEM prior to randomization (years)
Mean (SD) / Range
6.7 (6.08)
0.3 - 22.3
6.7 (5.70)
1.1 - 19.8
Duration of 3,4-DAP treatment at entry (years)
Mean (SD) / Range
5.5 (4.92)
0.3 - 18.3
6.2 (5.30)
0.7 - 18.9
Total Daily Dose of 3,4-DAP at entry (mg)
Mean (SD) / Range
74.7 (22.26)
30 - 100
76.4 (19.46)
35 - 100
LEM treatment before and during study
3,4-DAP + PB, N (%)
3,4-DAP, N (%)
3,4-DAP + PB + IM, N (%)
3,4-DAP + IM, N (%)
11 (61.1%)
0 (0.0%)
4 (22.2%)
3 (16.7%)
9 (64.3%)
1 (7.1%)
2 (14.2%)
2 (14.2%)
VGCC Ab, voltage-gated calcium channel antibodies
PB, pyridostigmine bromide; IM, immunomodulators/immunosuppressants
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Table 2. Primary and Secondary Efficacy Endpoints: Change in the final 3TUG Times and W-
SAS upon withdrawal of study drug
Study Group
Taper Continuous
to Placebo 3,4-DAP base
N=18 N=14
3TUG Change
N (%)
No Change or Faster
>30% Slower
5 (27.8%)
13 (72.2%)
14 (100%)
0 (0%)
P<0.0001*
Final W-SAS
N (%)
Much Much Weaker (-3)
Much Weaker (-2)
Somewhat Weaker (-1)
About the Same (0)
Somewhat Stronger (+1)
Much Stronger (+2)
Much Much Stronger (+3)
10 (55.6%)
6 (33.3%)
1 (5.6%)
1 (5.6%)
0 (0.0%)
0 (0.0%)
0 (0.0%)
1 (7.1%)
1 (7.1%)
1 (7.1%)
9 (64.3%)
1 (7.1%)
1 (7.1%)
0 (0.0%)
P<0.0001†
*, P value based on Fisher's Exact Test
†, P value based on CMH test for categorical data
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Abbreviations
3,4-DAP 3,4-diaminopyridine base
3TUG triple timed up and go test
Ab Antibodies
ACh Acetylcholine
AE adverse event
ANCOVA analysis of covariance
CMAP compound muscle action potential
CMH Cochrane-Mantel-Haenszel statistic
CONSORT Consolidated Standards of Reporting Trials
DAPPER Diaminopyridine (DAP) Prospective Efficacy Research
ECG electrocardiogram
IM immunomodulators/immunosuppressants
LEFS Lower extremity function scale
LEM Lambert-Eaton Myasthenia
PB pyridostigmine bromide
QMG Quantitative Myasthenia Gravis score
QTcF electrocardiographic QT interval with Fridericia's correction
TDD total daily dose
TEAE treatment-emergent adverse event
VGCC voltage-gated calcium channels
W-SAS LEM-related weakness self-assessment scale
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Figures
Figure 1. Study design schematic. See text for details.
Figure 2. CONSORT diagram
Figure 3. Percent change from baseline in 3TUG at 2 hours after dosing vs time, by treatment
group.
M: Morning; A: Afternoon; E: Evening.
* P-value <0.05; ** P-value <0.01; *** P-value <0.001. P-value is based on the one-way
ANCOVA model, with the baseline 3TUGs as the covariate.
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Figure 1. Study design schematic. See text for details.
198x111mm (220 x 220 DPI)
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Figure 2. CONSORT diagram
215x279mm (200 x 200 DPI)
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Figure 3. Percent change from baseline in 3TUG at 2 hours after dosing vs time, by treatment group. M: Morning; A: Afternoon; E: Evening.
* P-value <0.05; ** P-value <0.01; *** P-value <0.001. P-value is based on the one-way ANCOVA model,
with the baseline 3TUGs as the covariate.
152x114mm (96 x 96 DPI)
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